Abstract

The polyglutamate derivatives of antifolates have been established as being a major determinant in the therapeutic efficiency of this class of antitumo agents. The formation of these derivatives has been characterized in a number of transformed cell lines and with isolated folypolyglutamate synthetase. In contrast, the process of cleavage of these y-glutamyl derivatives has not yet been evaluated in sufficient depth or detail. The focus of this study is the enzyme that catalyzes this process, y-glutamyl hydrolase (GH). Studies in the previous grant period have established a number of features about this enzyme: 1) it is a glycoprotein (Mr-55 kDa) with a peptide Mr of 33kDa, 2) it is primarily a secreted enzyme (in all tumor cells tested) whose primary cellular location is the lysosome, 3) an intracellular elevation in its activity is a mechanism of acquired drug resistance, 4) its elevation has a more profound effect in diminishing cellular antifolate polyglutamates than folyl polyglutamates, and 5) a cDNA for GH from rat hepatoma has been cloned and characterized and the deduced amino acid sequence established. A detailed evaluation of GH will be made in order to establish its role in the pharmacology of the antifolat including 1) further studies on GH gene and factors that alter its expressi , 2) the use of site directed mutagenesis and detailed physical and biochemical analysis to understand the structure of the glycoprotein and it mechanism of action, 3) determining the mechanism of alteration in enzyme activity in acquired drug resistance and in response to insulin and other perturbations in tissue culture conditions, 4) evaluating the cytolocalizat n of GH by microscopy using polyclonal antibodies and investigating its cellular trafficking, and 5) using molecular methodology to enhance or inhibit GH levels in cells and evaluate the outcome in terms of the effect antifolate activity and polyglutamylation, GH function and folate growth dependence. These investigations will be conducted to determine if GH can be exploited as a target or if the modification of its function can be util ed to enhance the therapeutic selectivity of the antifolates. Lastly, the secretion of GH will be examined in detail in order to understand its biological and pharmacological significance and to develop the tools to determine its potential as a diagnostic marker.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA025933-19
Application #
2856200
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Forry-Schaudies, Suzanne L
Project Start
1979-07-01
Project End
2000-12-31
Budget Start
1999-01-01
Budget End
2000-12-31
Support Year
19
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Wadsworth Center
Department
Type
DUNS #
110521739
City
Menands
State
NY
Country
United States
Zip Code
12204

  Publications

Yin, Dezhong; Galivan, John; Ao, Wei et al. (2003) Characterization of the human gamma-glutamyl hydrolase promoter and its gene expression in human tissues and cancer cell lines. Gene 312:281-8
Chave, Karen J; Ryan, Thomas J; Chmura, Stacey E et al. (2003) Identification of single nucleotide polymorphisms in the human gamma-glutamyl hydrolase gene and characterization of promoter polymorphisms. Gene 319:167-75
Cole, P D; Kamen, B A; Gorlick, R et al. (2001) Effects of overexpression of gamma-Glutamyl hydrolase on methotrexate metabolism and resistance. Cancer Res 61:4599-604
Sanchez-Alcazar, J A; Khodjakov, A; Schneider, E (2001) Anticancer drugs induce increased mitochondrial cytochrome c expression that precedes cell death. Cancer Res 61:1038-44
Sanchez-Alcazar, J A; Schneider, E; Martinez, M A et al. (2000) Tumor necrosis factor-alpha increases the steady-state reduction of cytochrome b of the mitochondrial respiratory chain in metabolically inhibited L929 cells. J Biol Chem 275:13353-61
Galivan, J; Ryan, T J; Chave, K et al. (2000) Glutamyl hydrolase. pharmacological role and enzymatic characterization. Pharmacol Ther 85:207-15
Chave, K J; Auger, I E; Galivan, J et al. (2000) Molecular modeling and site-directed mutagenesis define the catalytic motif in human gamma -glutamyl hydrolase. J Biol Chem 275:40365-70
Sanchez-Alcazar, J A; Ault, J G; Khodjakov, A et al. (2000) Increased mitochondrial cytochrome c levels and mitochondrial hyperpolarization precede camptothecin-induced apoptosis in Jurkat cells. Cell Death Differ 7:1090-100
Volk, E L; Rohde, K; Rhee, M et al. (2000) Methotrexate cross-resistance in a mitoxantrone-selected multidrug-resistant MCF7 breast cancer cell line is attributable to enhanced energy-dependent drug efflux. Cancer Res 60:3514-21
Galivan, J; Ryan, T; Rhee, M et al. (1999) Glutamyl hydrolase: properties and pharmacologic impact. Semin Oncol 26:33-7

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